Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo

Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo

Apolipoprotein E (apoE) is an important determinant for the uptake of triglyceride-rich emulsions and lipoproteins by the liver, and exerts affinity for both the LDL receptor (LDLr) and a distinct liver-specific recognition site. Our current aim was to assess the mechanism underlying the receptor-sp...

Full description

Bibliographic Details
Main Authors: P C Rensen, N Herijgers, M H Netscher, S C Meskers, M van Eck, T J van Berkel
Format: Article
Language:English
Published: Elsevier 1997-06-01
Series:Journal of Lipid Research
Online Access:http://www.sciencedirect.com/science/article/pii/S002222752037190X
id doaj-79801058b02645d783b6e368aa44fba6
record_format Article
spelling doaj-79801058b02645d783b6e368aa44fba62021-04-26T05:47:50ZengElsevierJournal of Lipid Research0022-22751997-06-0138610701084Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivoP C Rensen0N Herijgers1M H Netscher2S C Meskers3M van Eck4T J van Berkel5Division of Biopharmaceutics, Leiden-Amsterdam Center for Drug Research, University of Leiden, Sylvius Laboratories, The Netherlands.Division of Biopharmaceutics, Leiden-Amsterdam Center for Drug Research, University of Leiden, Sylvius Laboratories, The Netherlands.Division of Biopharmaceutics, Leiden-Amsterdam Center for Drug Research, University of Leiden, Sylvius Laboratories, The Netherlands.Division of Biopharmaceutics, Leiden-Amsterdam Center for Drug Research, University of Leiden, Sylvius Laboratories, The Netherlands.Division of Biopharmaceutics, Leiden-Amsterdam Center for Drug Research, University of Leiden, Sylvius Laboratories, The Netherlands.Division of Biopharmaceutics, Leiden-Amsterdam Center for Drug Research, University of Leiden, Sylvius Laboratories, The Netherlands.Apolipoprotein E (apoE) is an important determinant for the uptake of triglyceride-rich emulsions and lipoproteins by the liver, and exerts affinity for both the LDL receptor (LDLr) and a distinct liver-specific recognition site. Our current aim was to assess the mechanism underlying the receptor-specificity of apoE-carrying lipoproteins. Triglyceride-rich emulsions were synthesized, with mean sizes of 50, 80, and 150 nm. These fractions efficiently acquired apoE from rat serum, and were processed by LPL in vivo with a similar efficiency. Upon injection of the [5H]cholesteryl oleate-labeled emulsions into rats, the liver association rate was positively correlated with particle size (24 +/- 2%, 54 +/- 1%, and 64 +/- 3% of the injected dose at 20 min after injection, respectively) and the liver uptake was predominantly exerted by parenchymal cells. The role of the LDLr in emulsion clearance was established in wild-type versus LDLr knockout mice. In the absence of the LDLr, an 8-fold increased serum half-life was observed for the small emulsion, concomitant with a 6- and 15-fold decreased uptake by the liver and adrenals at 60 min after injection, respectively. In contrast, the in vivo behavior of the large emulsion was independent of the LDLr. Both the ratio of apoE:C on the emulsions upon serum incubation and the alpha-helical content of apoE were inversely correlated with particle size, indicating that these factors may be involved in the emulsion size-dependent receptor specificity in vivo. It is concluded that the contribution of the LDLr to the apoE-mediated clearance of emulsions by the liver and adrenals strongly increases with decreasing particle size, while large particles initially associate with a distinct liver-specific recognition site. As these emulsions mimic chylomicrons, we anticipate that the apoE-dependent metabolic behavior of chylomicrons (remnants) is largely dependent on their size.http://www.sciencedirect.com/science/article/pii/S002222752037190X
collection DOAJ
language English
format Article
sources DOAJ
author P C Rensen
N Herijgers
M H Netscher
S C Meskers
M van Eck
T J van Berkel
spellingShingle P C Rensen
N Herijgers
M H Netscher
S C Meskers
M van Eck
T J van Berkel
Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo
Journal of Lipid Research
author_facet P C Rensen
N Herijgers
M H Netscher
S C Meskers
M van Eck
T J van Berkel
author_sort P C Rensen
title Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo
title_short Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo
title_full Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo
title_fullStr Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo
title_full_unstemmed Particle size determines the specificity of apolipoprotein E-containing triglyceride-rich emulsions for the LDL receptor versus hepatic remnant receptor in vivo
title_sort particle size determines the specificity of apolipoprotein e-containing triglyceride-rich emulsions for the ldl receptor versus hepatic remnant receptor in vivo
publisher Elsevier
series Journal of Lipid Research
issn 0022-2275
publishDate 1997-06-01
description Apolipoprotein E (apoE) is an important determinant for the uptake of triglyceride-rich emulsions and lipoproteins by the liver, and exerts affinity for both the LDL receptor (LDLr) and a distinct liver-specific recognition site. Our current aim was to assess the mechanism underlying the receptor-specificity of apoE-carrying lipoproteins. Triglyceride-rich emulsions were synthesized, with mean sizes of 50, 80, and 150 nm. These fractions efficiently acquired apoE from rat serum, and were processed by LPL in vivo with a similar efficiency. Upon injection of the [5H]cholesteryl oleate-labeled emulsions into rats, the liver association rate was positively correlated with particle size (24 +/- 2%, 54 +/- 1%, and 64 +/- 3% of the injected dose at 20 min after injection, respectively) and the liver uptake was predominantly exerted by parenchymal cells. The role of the LDLr in emulsion clearance was established in wild-type versus LDLr knockout mice. In the absence of the LDLr, an 8-fold increased serum half-life was observed for the small emulsion, concomitant with a 6- and 15-fold decreased uptake by the liver and adrenals at 60 min after injection, respectively. In contrast, the in vivo behavior of the large emulsion was independent of the LDLr. Both the ratio of apoE:C on the emulsions upon serum incubation and the alpha-helical content of apoE were inversely correlated with particle size, indicating that these factors may be involved in the emulsion size-dependent receptor specificity in vivo. It is concluded that the contribution of the LDLr to the apoE-mediated clearance of emulsions by the liver and adrenals strongly increases with decreasing particle size, while large particles initially associate with a distinct liver-specific recognition site. As these emulsions mimic chylomicrons, we anticipate that the apoE-dependent metabolic behavior of chylomicrons (remnants) is largely dependent on their size.
url http://www.sciencedirect.com/science/article/pii/S002222752037190X
work_keys_str_mv AT pcrensen particlesizedeterminesthespecificityofapolipoproteinecontainingtriglyceriderichemulsionsfortheldlreceptorversushepaticremnantreceptorinvivo
AT nherijgers particlesizedeterminesthespecificityofapolipoproteinecontainingtriglyceriderichemulsionsfortheldlreceptorversushepaticremnantreceptorinvivo
AT mhnetscher particlesizedeterminesthespecificityofapolipoproteinecontainingtriglyceriderichemulsionsfortheldlreceptorversushepaticremnantreceptorinvivo
AT scmeskers particlesizedeterminesthespecificityofapolipoproteinecontainingtriglyceriderichemulsionsfortheldlreceptorversushepaticremnantreceptorinvivo
AT mvaneck particlesizedeterminesthespecificityofapolipoproteinecontainingtriglyceriderichemulsionsfortheldlreceptorversushepaticremnantreceptorinvivo
AT tjvanberkel particlesizedeterminesthespecificityofapolipoproteinecontainingtriglyceriderichemulsionsfortheldlreceptorversushepaticremnantreceptorinvivo
_version_ 1721508672109019136

Similar Items